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在传入神经依赖的神经元存活关键期,小鼠蜗腹侧核神经元中自发性微小兴奋性突触后电流的发育。

Development of spontaneous miniature EPSCs in mouse AVCN neurons during a critical period of afferent-dependent neuron survival.

作者信息

Lu Yong, Harris Julie A, Rubel Edwin W

机构信息

Virginia Merrill Bloedel Hearing Research Center, University of Washington, Box 357923, Seattle, WA 98195, USA.

出版信息

J Neurophysiol. 2007 Jan;97(1):635-46. doi: 10.1152/jn.00915.2006. Epub 2006 Nov 1.

Abstract

During a critical period prior to hearing onset, cochlea ablation leads to massive neuronal death in the mouse anteroventral cochlear nucleus (AVCN), where cell survival is believed to depend on glutamatergic input. We investigated the development of spontaneous miniature excitatory postsynaptic currents (mEPSCs) in AVCN neurons using whole cell patch-clamp techniques during [postnatal day 7 (P7)] and after (P14, P21) this critical period. We also examined the effects of unilateral cochlea ablation on mEPSC development. The two main AVCN neuron types, bushy and stellate cells, were distinguished electrophysiologically. Bushy cell mEPSCs became more frequent and faster between P7 and P14/P21 but with little change in amplitude. Dendritic filtering of mEPSCs was not detected as indicated by the lack of correlation between 10 and 90% rise times and decay time constants. Seven days after cochlea ablation at P7 or P14, mEPSCs in surviving bushy cells were similar to controls, except that rise and decay times were positively correlated (R = 0.31 and 0.14 for surgery at P7 and P14, respectively). Consistent with this evidence for a shift of synaptic activity from the somata to the dendrites, SV2 staining (a synaptic vesicle marker) forms a ring around somata of control but not experimental bushy cells. In contrast, mEPSCs of stellate cells showed few significant changes over these ages with or without cochlea ablation. Taken together, mEPSCs in mouse AVCN bushy cells show dramatic developmental changes across this critical period, and cochlea ablation may lead to the emergence of excitatory synaptic inputs impinging on bushy cell dendrites.

摘要

在听力开始之前的关键时期,耳蜗切除会导致小鼠前腹侧耳蜗核(AVCN)中大量神经元死亡,据信该区域的细胞存活依赖于谷氨酸能输入。我们使用全细胞膜片钳技术,在出生后第7天(P7)以及该关键时期之后(P14、P21),研究了AVCN神经元中自发微小兴奋性突触后电流(mEPSCs)的发育情况。我们还研究了单侧耳蜗切除对mEPSC发育的影响。通过电生理方法区分了AVCN的两种主要神经元类型,即浓密型和星型细胞。在P7至P14/P21期间,浓密型细胞的mEPSCs变得更加频繁且速度更快,但幅度变化不大。10%至90%上升时间与衰减时间常数之间缺乏相关性,这表明未检测到mEPSCs的树突滤波现象。在P7或P14进行耳蜗切除7天后,存活的浓密型细胞中的mEPSCs与对照组相似,只是上升和衰减时间呈正相关(P7和P14手术时的相关系数分别为0.31和0.14)。与突触活动从胞体转移到树突的这一证据一致,SV2染色(一种突触囊泡标记物)在对照浓密型细胞的胞体周围形成一个环,而在实验性浓密型细胞中则没有。相比之下,无论有无耳蜗切除,星型细胞的mEPSCs在这些年龄段几乎没有显著变化。综上所述,小鼠AVCN浓密型细胞中的mEPSCs在这个关键时期呈现出显著的发育变化,耳蜗切除可能导致兴奋性突触输入出现在浓密型细胞的树突上。

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